Learning objectives To elucidate the potential advantages of albumin administration in severe sepsis. Introduction Albumin accounts for 80% of colloid osmotic pressure and its domains determine the binding properties for several endogenous molecules and drugs. Moreover plasma albumin concentration is a powerful dose-dependent predictor of mortality. Three metanalysis found albumin administration harmful, neutral and advantageous. The subgroup analysis of SAFE study showed a beneficial trend in septic patients treated with albumin and unfavourable trend in trauma patients with brain injury. For a given reached intravascular volume this effect must be similar for crystalloids, artificial colloids and albumin. Consequently, possible advantages of albumin should be due to a lower complication occurrence and/or to non-oncotic functions. In contrast, albumin did not show these complications and showed antioxidant properties and buffer-effect on nitric oxide metabolism. The results obtained in the hepatorenal syndrome and the favourable trend in sepsis indirectly suggest that the albumin non-oncotic functions are relevant; however, ad hoc studies must specifically address this issue. Methods Multicenter (100 italian ICU) randomized clinical trial on 1818 patients with severe sepsis. Patients randomly received either 20% albumin and crystalloids or crystalloids alone for volume replacement until ICU discharge or 28 days after randomization. Primary outcomes were survival at 28 and 90 days. Discussion The addition of albumin to crystalloids during both early volume resuscitation and the first 28 days of treatment to correct hypoalbuminemia is safe, but does not bring forth a survival advantage as compared to the administration of crystalloids alone over a follow-up period of 28 and 90 days. A post-hoc analysis of the 1303 patients with severe septic shock showed a significantly lower 90-day mortality in the Albumin group as compared to the Crystalloid group. Conversely, in patients treated with albumin with severe sepsis without septic shock mortality rate appeared higher although not significantly different. Conclusions In conclusion, the use of albumin in addition to crystalloids in patients with severe sepsis during early resuscitation and ICU stay to correct hypoalbuminemia does not provide survival benefit at 90 days over the use of crystalloids alone, despite improvements in hemodynamics. The clinical benefit of albumin in the subgroup of patients with septic shock deserves further confirmation.
The Albios study: resuscitation and/or supplementation / L. Gattinoni. ((Intervento presentato al 34. convegno International Symposium on Intensive Care and Emergency Medicine tenutosi a Brussels nel 2014.
The Albios study: resuscitation and/or supplementation
L. Gattinoni
2014
Abstract
Learning objectives To elucidate the potential advantages of albumin administration in severe sepsis. Introduction Albumin accounts for 80% of colloid osmotic pressure and its domains determine the binding properties for several endogenous molecules and drugs. Moreover plasma albumin concentration is a powerful dose-dependent predictor of mortality. Three metanalysis found albumin administration harmful, neutral and advantageous. The subgroup analysis of SAFE study showed a beneficial trend in septic patients treated with albumin and unfavourable trend in trauma patients with brain injury. For a given reached intravascular volume this effect must be similar for crystalloids, artificial colloids and albumin. Consequently, possible advantages of albumin should be due to a lower complication occurrence and/or to non-oncotic functions. In contrast, albumin did not show these complications and showed antioxidant properties and buffer-effect on nitric oxide metabolism. The results obtained in the hepatorenal syndrome and the favourable trend in sepsis indirectly suggest that the albumin non-oncotic functions are relevant; however, ad hoc studies must specifically address this issue. Methods Multicenter (100 italian ICU) randomized clinical trial on 1818 patients with severe sepsis. Patients randomly received either 20% albumin and crystalloids or crystalloids alone for volume replacement until ICU discharge or 28 days after randomization. Primary outcomes were survival at 28 and 90 days. Discussion The addition of albumin to crystalloids during both early volume resuscitation and the first 28 days of treatment to correct hypoalbuminemia is safe, but does not bring forth a survival advantage as compared to the administration of crystalloids alone over a follow-up period of 28 and 90 days. A post-hoc analysis of the 1303 patients with severe septic shock showed a significantly lower 90-day mortality in the Albumin group as compared to the Crystalloid group. Conversely, in patients treated with albumin with severe sepsis without septic shock mortality rate appeared higher although not significantly different. Conclusions In conclusion, the use of albumin in addition to crystalloids in patients with severe sepsis during early resuscitation and ICU stay to correct hypoalbuminemia does not provide survival benefit at 90 days over the use of crystalloids alone, despite improvements in hemodynamics. The clinical benefit of albumin in the subgroup of patients with septic shock deserves further confirmation.
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